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作为药物纳米载体的非离子表面活性剂囊泡:多尺度pH依赖性结构响应

Niosomes as Drug Nanovectors: Multiscale pH-Dependent Structural Response.

作者信息

Marianecci Carlotta, Di Marzio Luisa, Del Favero Elena, Cantù Laura, Brocca Paola, Rondelli Valeria, Rinaldi Federica, Dini Luciana, Serra Antonio, Decuzzi Paolo, Celia Christian, Paolino Donatella, Fresta Massimo, Carafa Maria

机构信息

Department of Drug Chemistry and Technology, University of Rome "Sapienza" , 00185 Rome, Italy.

Department of Pharmacy, University of Chieti - Pescara "G d'Annunzio" , 66100 Chieti - Pescara, Italy.

出版信息

Langmuir. 2016 Feb 9;32(5):1241-9. doi: 10.1021/acs.langmuir.5b04111. Epub 2016 Jan 19.

Abstract

The use of nanocarriers, which respond to different stimuli controlling their physicochemical properties and biological responsivness, shows a growing interest in pharmaceutical science. The stimuli are activated by targeting tissues and biological compartments, e.g., pH modification, temperature, redox condition, enzymatic activity, or can be physically applied, e.g., a magnetic field and ultrasound. pH modification represents the easiest method of passive targeting, which is actually used to accumulate nanocarriers in cells and tissues. The aim of this paper was to physicochemically characterize pH-sensitive niosomes using different experimental conditions and demonstrate the effect of surfactant composition on the supramolecular structure of niosomes. In this attempt, niosomes, made from commercial (Tween21) and synthetic surfactants (Tween20 derivatives), were physicochemically characterized by using different techniques, e.g., transmission electron microscopy, Raman spectroscopy, and small-angle X-ray scattering. The changes of niosome structure at different pHs depend on surfactants, which can affect the supramolecular structure of colloidal nanocarriers and their potential use both in vitro and in vivo. At pH 7.4, the shape and structure of niosomes have been maintained; however, niosomes show some differences in terms of bilayer thicknesses, water penetration, membrane coupling, and cholesterol dispersion. The acid pH (5.5) can increase the bilayer fluidity, and affect the cholesterol depletion. In fact, Tween21 niosomes form large vesicles with lower curvature radius at acid pH; while Tween20-derivative niosomes increase the intrachain mobility within a more interchain correlated membrane. These results demonstrate that the use of multiple physicochemical procedures provides more information about supramolecular structures of niosomes and improves the opportunity to deeply investigate the effect of stimuli responsiveness on the niosome structure.

摘要

对能够响应不同刺激以控制其物理化学性质和生物学响应性的纳米载体的应用,在药学领域正展现出越来越浓厚的兴趣。这些刺激可通过靶向组织和生物区室来激活,例如pH值改变、温度、氧化还原条件、酶活性,或者也可以通过物理方式施加,例如磁场和超声波。pH值改变是被动靶向的最简单方法,实际上它被用于使纳米载体在细胞和组织中积累。本文的目的是在不同实验条件下对pH敏感的非离子表面活性剂囊泡进行物理化学表征,并证明表面活性剂组成对非离子表面活性剂囊泡超分子结构的影响。在这一尝试中,由商用(吐温21)和合成表面活性剂(吐温20衍生物)制成的非离子表面活性剂囊泡,通过使用不同技术进行了物理化学表征,例如透射电子显微镜、拉曼光谱和小角X射线散射。不同pH值下非离子表面活性剂囊泡结构的变化取决于表面活性剂,这会影响胶体纳米载体的超分子结构及其在体外和体内的潜在用途。在pH 7.4时,非离子表面活性剂囊泡的形状和结构得以维持;然而,非离子表面活性剂囊泡在双层厚度、水渗透、膜偶联和胆固醇分散方面存在一些差异。酸性pH(5.5)可增加双层流动性,并影响胆固醇的消耗。事实上,吐温21非离子表面活性剂囊泡在酸性pH下形成曲率半径较小的大囊泡;而吐温20衍生物非离子表面活性剂囊泡则增加了在链间相关性更高的膜内的链内流动性。这些结果表明,使用多种物理化学方法可提供更多关于非离子表面活性剂囊泡超分子结构的信息,并增加深入研究刺激响应性对非离子表面活性剂囊泡结构影响的机会。

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